Emerging research suggests that the timing of environmental factors in the presence of genetic predispositions has influenced the increase in autism spectrum disorders over the past several decades. A review of the medical literature suggests that autism may be impacted by environmental toxicants, breastfeeding duration, gut flora composition, nutritional status, acetaminophen use, vaccine practices and use of antibiotics and/or frequency of infections. The author reports her retrospective clinical research in a general pediatric practice (Advocates for Children), which shows a modest trend toward lower prevalence of autism than her previous pediatric practice or recent CDC data. Out of 294 general pediatrics patients followed since 2005 there were zero new cases of autism (p value 0.014). Given the prevalence of autism for that cohort of 1 in 50 children in the United States, it is important to consider implementing strategies in primary care practice that could potentially modify environmental factors or affect the timing of environmental triggers contributing to autism.

Abstract
There is a compelling argument that the occurrence of regressive autism is attributable to genetic and chromosomal abnormalities, arising from the overuse of vaccines, which subsequently affects the stability and function of the autonomic nervous system and physiological systems. That sense perception is linked to the autonomic nervous system and the function of the physiological systems enables us to examine the significance of autistic symptoms from a systemic perspective. Failure of the excretory system influences elimination of heavy metals and facilitates their accumulation and subsequent manifestation as neurotoxins: the long-term consequences of which would lead to neurodegeneration, cognitive and developmental problems. It may also influence regulation of neural hyperthermia. This article explores the issues and concludes that sensory dysfunction and systemic failure, manifested as autism, is the inevitable consequence arising from subtle DNA alteration and consequently from the overuse of vaccines.

Case 3. Richard M. was referred to the Johns Hopkins Hospital on February 5, 1941, at 3 years, 3 months of age, with the complaint of deafness because he didnot talk and did not respond to questions.
Following smallpox vaccination at 12 months, he had an attack of diarrhea and fever, from which he recovered in somewhat less than a week
In september, 1940, the mother, in commenting on Richard’s failure to talk, remarked in her notes: I can’t be sure just when he stopped the imitation of wordssounds. It seems that he has gone backward mentally gradually for the last two years.
Richard M
November 1937 – Born
November 1938 – vaccinated with Smallpox vaccine
September 1940 – Mother reports developmental regression beginning approximately two years previously
February 1941 – Referred to Hopkins for evaluation
1943 – Becomes the third child to be described as autistic by Leo Kanner in his disorder defining paper, the first paper published on autism

VAXXED TV – Hib Vaccination: The Bigger Picture #PrayBig

My unvaccinated extremely healthy children

Read The Insert

HPV Gardasil vaccine injured my daughter

A Certain Brightness and Intelligence

Vaccines injured my boy

Vaccinations gave my son autism

4 month vaccinations killed my baby

I will never vaccinate my family again

Dr Jeremy Kobler

****************************************************

ONE FOR ISRAEL Ministry – Jewish Johnathan Ben-David forgave his killer and you would not believe why!!!

1 Corinthians 15 Authorized (King James) Version (AKJV)
1 Moreover, brethren, I declare unto you the gospel which I preached unto you, which also ye have received, and wherein ye stand;
2 by which also ye are saved, if ye keep in memory what I preached unto you, unless ye have believed in vain.
3 For I delivered unto you first of all that which I also received, how that Christ died for our sins according to the scriptures;
4 and that he was buried, and that he rose again the third day according to the scriptures:

Hebrews 6 Authorized (King James) Version (AKJV)
1 Therefore leaving the principles of the doctrine of Christ, let us go on unto perfection; not laying again the foundation of repentance from dead works, and of faith toward God,
2 of the doctrine of baptisms, and of laying on of hands, and of resurrection of the dead, and of eternal judgment.
3 And this will we do, if God permit.
4 For it is impossible for those who were once enlightened, and have tasted of the heavenly gift, and were made partakers of the Holy Ghost,
5 and have tasted the good word of God, and the powers of the world to come,
6 if they shall fall away, to renew them again unto repentance; seeing they crucify to themselves the Son of God afresh, and put him to an open shame.
7 For the earth which drinketh in the rain that cometh oft upon it, and bringeth forth herbs meet for them by whom it is dressed, receiveth blessing from God:
8 but that which beareth thorns and briers is rejected, and is nigh unto cursing; whose end is to be burned.

1 Who hath believed our report? and to whom is the arm of the Lord revealed?
2 For he shall grow up before him as a tender plant,and as a root out of a dry ground:he hath no form nor comeliness;and when we shall see him,there is no beauty that we should desire him.
3 He is despised and rejected of men;a man of sorrows, and acquainted with grief:and we hid as it were our faces from him;he was despised, and we esteemed him not.
4 Surely he hath borne our griefs,and carried our sorrows:yet we did esteem him stricken,smitten of God, and afflicted.
5 But he was wounded for our transgressions,he was bruised for our iniquities:the chastisement of our peace was upon him;and with his stripes we are healed.
6 All we like sheep have gone astray;we have turned every one to his own way;and the Lord hath laid on him the iniquity of us all.
7 He was oppressed, and he was afflicted,yet he opened not his mouth:he is brought as a lamb to the slaughter,and as a sheep before her shearers is dumb,so he openeth not his mouth.
8 He was taken from prison and from judgment:and who shall declare his generation? for he was cut off out of the land of the living:for the transgression of my people was he stricken.
9 And he made his grave with the wicked,and with the rich in his death;because he had done no violence,neither was any deceit in his mouth.
10 Yet it pleased the Lord to bruise him;he hath put him to grief:when thou shalt make his soul an offering for sin,he shall see his seed, he shall prolong his days,and the pleasure of the Lord shall prosper in his hand.
11 He shall see of the travail of his soul, and shall be satisfied:by his knowledge shall my righteous servant justify many;for he shall bear their iniquities.
12 Therefore will I divide him a portion with the great,and he shall divide the spoil with the strong;because he hath poured out his soul unto death:and he was numbered with the transgressors;and he bare the sin of many,and made intercession for the transgressors.

A study published in the Journal of Toxicology and Environmental Health determined that mercury exposure can induce immune, sensory, neurological, motor and behavioural dysfunctions similar to traits defining or associated with ASDs. Based upon differential diagnoses, 8 of 9 patients examined were exposed to significant mercury from Thimerosal-containing vaccine preparations during their fetal/infant developmental periods. These previously normal developing children suffered mercury encephalopathies that manifested with clinical symptoms consistent with regressive ASDs. Evidence for mercury intoxication should be considered in the differential diagnosis as contributing to some regressive ASDs.

US National Library of Medicine
National Institutes of Health – May 2007

Abstract
Impairments in social relatedness and communication, repetitive behaviors, and stereotypic abnormal movement patterns characterize autism spectrum disorders (ASDs). It is clear that while genetic factors are important to the pathogenesis of ASDs, mercury exposure can induce immune, sensory, neurological, motor, and behavioral dysfunctions similar to traits defining or associated with ASDs. The Institutional Review Board of the Institute for Chronic Illnesses (Office for Human Research Protections, U.S. Department of Health and Human Services, IRB number IRB00005375) approved the present study. A case series of nine patients who presented to the Genetic Centers of America for a genetic/developmental evaluation are discussed. Eight of nine patients (one patient was found to have an ASD due to Rett’s syndrome) (a) had regressive ASDs; (b) had elevated levels of androgens; (c) excreted significant amounts of mercury post chelation challenge; (d) had biochemical evidence of decreased function in their glutathione pathways; (e) had no known significant mercury exposure except from Thimerosal-containing vaccines/Rho(D)-immune globulin preparations; and (f) had alternate causes for their regressive ASDs ruled out. There was a significant dose-response relationship between the severity of the regressive ASDs observed and the total mercury dose children received from Thimerosal-containing vaccines/Rho (D)-immune globulin preparations. Based upon differential diagnoses, 8 of 9 patients examined were exposed to significant mercury from Thimerosal-containing biologic/vaccine preparations during their fetal/infant developmental periods, and subsequently, between 12 and 24 mo of age, these previously normally developing children suffered mercury toxic encephalopathies that manifested with clinical symptoms consistent with regressive ASDs. Evidence for mercury intoxication should be considered in the differential diagnosis as contributing to some regressive ASDs.

A study conducted by the Department of Obstetrics and Gynaecology at University of Pittsburgh’s School of Medicine showed that Macaques are commonly used in pre-clinical vaccine safety testing. Collective Evolution does not support animals testing, we feel there is a large amount of evidence and research that already indicated the links to vaccines in which some animals have been used to illustrate. The objective of this study was to compare early infant cognition and behaviour with amygdala size and opioid binding in rhesus macaques receiving the recommended childhood vaccines. The animal model, which examines for the first time, behavioural, functional and neuromorphometric consequences of the childhood vaccine regimen, mimics certain neurological abnormalities of autism. These findings raise important safety issues while providing a potential model for examining aspects of causation and disease pathogenesis in acquired disorders of behaviour and development.

Abstract
This longitudinal, case-control pilot study examined amygdala growth in rhesus macaque infants receiving the complete US childhood vaccine schedule (1994-1999). Longitudinal structural and functional neuroimaging was undertaken to examine central effects of the vaccine regimen on the developing brain. Vaccine-exposed and saline-injected control infants underwent MRI and PET imaging at approximately 4 and 6 months of age, representing two specific timeframes within the vaccination schedule. Volumetric analyses showed that exposed animals did not undergo the maturational changes over time in amygdala volume that was observed in unexposed animals. After controlling for left amygdala volume, the binding of the opioid antagonist [11C]diprenorphine (DPN) in exposed animals remained relatively constant over time, compared with unexposed animals, in which a significant decrease in [11C]DPN binding occurred. These results suggest that maturational changes in amygdala volume and the binding capacity of [11C]DPN in the amygdala was significantly altered in infant macaques receiving the vaccine schedule. The macaque infant is a relevant animal model in which to investigate specific environmental exposures and structural/functional neuroimaging during neurodevelopment.

A study conducted by The George Washington University School of Public Health from the Department of Epidemiology and Biostatistics determined that significantly increased rate ratios were observed for autism and autism spectrum disorders as a result of exposure to mercury from Thimerosal-containing vaccines.

US National Library of Medicine
National Institutes of Health – Aug 2008

Young HA, Geier DA, Geier MR.
Author information
The George Washington University School of Public Health and Health Services, Department of Epidemiology and Biostatistics, United States.

Abstract
The study evaluated possible associations between neurodevelopmental disorders (NDs) and exposure to mercury (Hg) from Thimerosal-containing vaccines (TCVs) by examining the automated Vaccine Safety Datalink (VSD). A total of 278,624 subjects were identified in birth cohorts from 1990-1996 that had received their first oral polio vaccination by 3 months of age in the VSD. The birth cohort prevalence rate of medically diagnosed International Classification of Disease, 9th revision (ICD-9) specific NDs and control outcomes were calculated. Exposures to Hg from TCVs were calculated by birth cohort for specific exposure windows from birth-7 months and birth-13 months of age. Poisson regression analysis was used to model the association between the prevalence of outcomes and Hg doses from TCVs. Consistent significantly increased rate ratios were observed for autism, autism spectrum disorders, tics, attention deficit disorder, and emotional disturbances with Hg exposure from TCVs. By contrast, none of the control outcomes had significantly increased rate ratios with Hg exposure from TCVs. Routine childhood vaccination should be continued to help reduce the morbidity and mortality associated with infectious diseases, but efforts should be undertaken to remove Hg from vaccines. Additional studies should be conducted to further evaluate the relationship between Hg exposure and NDs.

1 Corinthians 15 Authorized (King James) Version (AKJV)
1 Moreover, brethren, I declare unto you the gospel which I preached unto you, which also ye have received, and wherein ye stand;
2 by which also ye are saved, if ye keep in memory what I preached unto you, unless ye have believed in vain.
3 For I delivered unto you first of all that which I also received, how that Christ died for our sins according to the scriptures;
4 and that he was buried, and that he rose again the third day according to the scriptures:

Hebrews 6 Authorized (King James) Version (AKJV)
1 Therefore leaving the principles of the doctrine of Christ, let us go on unto perfection; not laying again the foundation of repentance from dead works, and of faith toward God,
2 of the doctrine of baptisms, and of laying on of hands, and of resurrection of the dead, and of eternal judgment.
3 And this will we do, if God permit.
4 For it is impossible for those who were once enlightened, and have tasted of the heavenly gift, and were made partakers of the Holy Ghost,
5 and have tasted the good word of God, and the powers of the world to come,
6 if they shall fall away, to renew them again unto repentance; seeing they crucify to themselves the Son of God afresh, and put him to an open shame.
7 For the earth which drinketh in the rain that cometh oft upon it, and bringeth forth herbs meet for them by whom it is dressed, receiveth blessing from God:
8 but that which beareth thorns and briers is rejected, and is nigh unto cursing; whose end is to be burned.

A study conducted by the Department of Paediatrics at the University of Arkansas determined that thimerosal-induced cytotoxicity was associated with the depletion of intracellular glutathione (GSH) in both cell lines. The study outlines how many vaccines have been neurotoxic, especially to the developing brain. Depletion of GSH is commonly associated with autism. Although thimerosal has been removed from most children’s vaccines, it is still present in flu vaccines given to pregnant women, the elderly and to children in developing countries.

Abstract
Thimerosol is an antiseptic containing 49.5% ethyl mercury that has been used for years as a preservative in many infant vaccines and in flu vaccines. Environmental methyl mercury has been shown to be highly neurotoxic, especially to the developing brain. Because mercury has a high affinity for thiol (sulfhydryl (-SH)) groups, the thiol-containing antioxidant, glutathione (GSH), provides the major intracellular defense against mercury-induced neurotoxicity. Cultured neuroblastoma cells were found to have lower levels of GSH and increased sensitivity to thimerosol toxicity compared to glioblastoma cells that have higher basal levels of intracellular GSH. Thimerosal-induced cytotoxicity was associated with depletion of intracellular GSH in both cell lines. Pretreatment with 100 microM glutathione ethyl ester or N-acetylcysteine (NAC), but not methionine, resulted in a significant increase in intracellular GSH in both cell types. Further, pretreatment of the cells with glutathione ethyl ester or NAC prevented cytotoxicity with exposure to 15 microM Thimerosal. Although Thimerosal has been recently removed from most children’s vaccines, it is still present in flu vaccines given to pregnant women, the elderly, and to children in developing countries. The potential protective effect of GSH or NAC against mercury toxicity warrants further research as possible adjunct therapy to individuals still receiving Thimerosal-containing vaccinations.

A study conducted by the University of Texas Health Science Centre by the Department of Family and Community Medicine determined that for each 1,000 Ib of environmentally released mercury, there was a 43% increase in the rate of special education services and a 61% increase in the rate of autism. Researchers emphasized that further research was needed regarding the association between environmentally released mercury and developmental disorders such as autism.

Abstract
The association between environmentally released mercury, special education and autism rates in Texas was investigated using data from the Texas Education Department and the United States Environmental Protection Agency. A Poisson regression analysis adjusted for school district population size, economic and demographic factors was used. There was a significant increase in the rates of special education students and autism rates associated with increases in environmentally released mercury. On average, for each 1,000 lb of environmentally released mercury, there was a 43% increase in the rate of special education services and a 61% increase in the rate of autism. The association between environmentally released mercury and special education rates were fully mediated by increased autism rates. This ecological study suggests the need for further research regarding the association between environmentally released mercury and developmental disorders such as autism. These results have implications for policy planning and cost analysis.

A study published in the International Journal of Toxicology determined that in light of the biological plausibility of mercury’s role in neurodevelopment disorders, the present study provides further insight into one possible mechanism by which early mercury exposures could increase the risk of autism.

Abstract
Reported rates of autism have increased sharply in the United States and the United Kingdom. One possible factor underlying these increases is increased exposure to mercury through thimerosal-containing vaccines, but vaccine exposures need to be evaluated in the context of cumulative exposures during gestation and early infancy. Differential rates of postnatal mercury elimination may explain why similar gestational and infant exposures produce variable neurological effects. First baby haircut samples were obtained from 94 children diagnosed with autism using Diagnostic and Statistical Manual of Mental Disorders, 4th edition (DSM IV) criteria and 45 age- and gender-matched controls. Information on diet, dental amalgam fillings, vaccine history, Rho D immunoglobulin administration, and autism symptom severity was collected through a maternal survey questionnaire and clinical observation. Hair mercury levels in the autistic group were 0.47 ppm versus 3.63 ppm in controls, a significant difference. The mothers in the autistic group had significantly higher levels of mercury exposure through Rho D immunoglobulin injections and amalgam fillings than control mothers. Within the autistic group, hair mercury levels varied significantly across mildly, moderately, and severely autistic children, with mean group levels of 0.79, 0.46, and 0.21 ppm, respectively. Hair mercury levels among controls were significantly correlated with the number of the mothers’ amalgam fillings and their fish consumption as well as exposure to mercury through childhood vaccines, correlations that were absent in the autistic group. Hair excretion patterns among autistic infants were significantly reduced relative to control. These data cast doubt on the efficacy of traditional hair analysis as a measure of total mercury exposure in a subset of the population. In light of the biological plausibility of mercury’s role in neurodevelopmental disorders, the present study provides further insight into one possible mechanism by which early mercury exposures could increase the risk of autism.

1 Corinthians 15 Authorized (King James) Version (AKJV)
1 Moreover, brethren, I declare unto you the gospel which I preached unto you, which also ye have received, and wherein ye stand;
2 by which also ye are saved, if ye keep in memory what I preached unto you, unless ye have believed in vain.
3 For I delivered unto you first of all that which I also received, how that Christ died for our sins according to the scriptures;
4 and that he was buried, and that he rose again the third day according to the scriptures:

Hebrews 6 Authorized (King James) Version (AKJV)
1 Therefore leaving the principles of the doctrine of Christ, let us go on unto perfection; not laying again the foundation of repentance from dead works, and of faith toward God,
2 of the doctrine of baptisms, and of laying on of hands, and of resurrection of the dead, and of eternal judgment.
3 And this will we do, if God permit.
4 For it is impossible for those who were once enlightened, and have tasted of the heavenly gift, and were made partakers of the Holy Ghost,
5 and have tasted the good word of God, and the powers of the world to come,
6 if they shall fall away, to renew them again unto repentance; seeing they crucify to themselves the Son of God afresh, and put him to an open shame.
7 For the earth which drinketh in the rain that cometh oft upon it, and bringeth forth herbs meet for them by whom it is dressed, receiveth blessing from God:
8 but that which beareth thorns and briers is rejected, and is nigh unto cursing; whose end is to be burned.

EXCLUSIVE UNCUT video interview with ‘VAXXED’ producer Del Bigtree that was 99% censored by ABC World News Tonight!
———————————————————————–
THE GOVERNMENT HAS BEEN MURDERING INNOCENT PEOPLE WITH VACCINES FOR DECADES AND THEY ARE BEING EXPOSED BEFORE OUR VERY EYES!
TO ALL OF THE FREEDOM FIGHTERS OUT THERE WHO TIRELESSLY EXPOSE THE TRUTH IN THE FACE OF INCREDIBLE CRITICISM AND PROPAGANDA, KEEP UP THE GOOD WORK!
THE GOVERNMENT IS RUNNING SCARED!
WE ARE MARCHING ON TO VICTORY!
——————————————————————————
“We set out to make a movie, now we’re making history…
To watch every major newspaper tell people not to see a movie, a movie they had never seen, is an unprecedented moment in this country. When has that ever happened?
Every major newspaper is saying don’t go see a movie they haven’t watched themselves. What’s next, are they going to tell us to start burning books in the streets? We’ve never seen anything like this.
This is supposed to be a country based on freedom of expression, and our entire media that [claims to] represent speech and expression, is telling everybody to shut down free speech. Journalism is officially DEAD in America.
We have a whistleblower at the CDC who is still sitting at the CDC, an awarded scientist, who is being protected by whistleblower status, and the media is saying we are making things up. They say they’ve debunked the whistleblower, but you can’t debunk someone who hasn’t had his day in court, just like you can’t review a movie you haven’t seen.”
Learn more: http://www.naturalnews.com/053448_Del_Bigtree_VAXXED_docume…
——————–
We are facing massive censorship and we are under attack from every angle but WE WILL BE VICTORIOUS!
PLEASE LIKE, SHARE (ESPECIALLY TO GROUPS), AND COMMENT ON THIS POST!
WE WILL DEFEAT EVIL BY HAVING THE COURAGE TO EXPOSE IT!
Thank you for all of your support!

•Blood mercury levels were repeatedly measured from early pregnancy to 3 years.

•Autistic behaviors were assessed at 5 years with the Social Responsiveness Scale.

•Prenatal and early childhood mercury levels were associated with autistic behaviors.

Abstract

Background

Although mercury is an established neurotoxin, only few longitudinal studies have investigated the association between prenatal and early childhood mercury exposure and autistic behaviors.

Methods

We conducted a longitudinal cohort study using an ongoing prospective birth cohort initiated in 2006, wherein blood mercury levels were measured at early and late pregnancy; in cord blood; and at 2 and 3 years of age. We analyzed 458 mother-child pairs. Autistic behaviors were assessed using the Social Responsiveness Scale (SRS) at 5 years of age. Both continuous SRS T-scores and T-scores dichotomized by a score of ≥ 60 or < 60 were used as outcomes.

We found that blood mercury levels at late pregnancy and early childhood were associated with more autistic behaviors in children at 5 years of age. Further study on the long-term effects of mercury exposure is recommended.

Exposure to organic forms of mercury has the theoretical capacity to generate a range of immune abnormalities coupled with chronic nitro-oxidative stress seen in children with autism spectrum disorder (ASD). The paper discusses possible mechanisms explaining the neurotoxic effects of mercury and possible associations between mercury exposure and ASD subtypes. Environmental mercury is neurotoxic at doses well below the current reference levels considered to be safe, with evidence of neurotoxicity in children exposed to environmental sources including fish consumption and ethylmercury-containing vaccines. Possible neurotoxic mechanisms of mercury include direct effects on sulfhydryl groups, pericytes and cerebral endothelial cells, accumulation within astrocytes, microglial activation, induction of chronic oxidative stress, activation of immune-inflammatory pathways and impairment of mitochondrial functioning. (Epi-)genetic factors which may increase susceptibility to the toxic effects of mercury in ASD include the following: a greater propensity of males to the long-term neurotoxic effects of postnatal exposure and genetic polymorphisms in glutathione transferases and other glutathione-related genes and in selenoproteins. Furthermore, immune and inflammatory responses to immunisations with mercury-containing adjuvants are strongly influenced by polymorphisms in the human leukocyte antigen (HLA) region and by genes encoding effector proteins such as cytokines and pattern recognition receptors. Some epidemiological studies investigating a possible relationship between high environmental exposure to methylmercury and impaired neurodevelopment have reported a positive dose-dependent effect. Retrospective studies, on the other hand, reported no relationship between a range of ethylmercury-containing vaccines and chronic neuropathology or ASD. On the basis of these results, we would argue that more clinically relevant research is required to examine whether environmental mercury is associated with ASD or subtypes. Specific recommendations for future research are discussed.

Environmental factors have been implicated in the etiology of autism spectrum disorder (ASD); however, the role of heavy metals has not been fully defined. This study investigated whether blood levels of mercury, arsenic, cadmium, and lead of children with ASD significantly differ from those of age- and sex-matched controls. One hundred eighty unrelated children with ASD and 184 healthy controls were recruited. Data showed that the children with ASD had significantly (p < 0.001) higher levels of mercury and arsenic and a lower level of cadmium. The levels of lead did not differ significantly between the groups. The results of this study are consistent with numerous previous studies, supporting an important role for heavy metal exposure, particularly mercury, in the etiology of ASD. It is desirable to continue future research into the relationship between ASD and heavy metal exposure

Dr. Brownstein on CDC Corruption: “I am Tired of Writing About This – I See Patients Damaged by Vaccines”
CDC Whistleblower Case Three Years Later: Nothing Happening
by Dr. Brownstein’s
Holistic Medicine
I honestly cannot believe I am still writing about this. It was three years ago that a senior CDC scientist, Dr. William Thompson, claimed whistleblower protection after he issued a statement that he and his fellow colleagues altered, hid, and threw out data that showed a direct association between the MMR vaccine and autism.

CDC Whistleblower Case Three Years Later: Nothing Happening
I honestly cannot believe I am still writing about this. It was three years ago that a senior CDC scientist, Dr. William Thompson, claimed whistleblower protection after he issued a statement that he and his fellow colleagues altered, hid, and threw out data that showed a direct association between the MMR vaccine and autism. In August, 2014, I wrote in a blog post, “Now, there may be proof that the CDC not only knew about the link between the MMR vaccine and autism but they changed the data in a landmark 2004 study to hide the damning data. What did the heads of the CDC do? They altered the data and reported in 2004 (1) that there was no association between autism and the MMR vaccine. Who wrote this article? William Thompson, PhD, the whistleblower, was one of the authors of that 2004 study. He is reported to be suffering with regret and remorse over the damage that has been done to our children over the last ten years.”
The data that was altered showed a whopping 240% increase in autism cases among African American males who received the MMR vaccine before 36 months of age. Furthermore, there was a 69% increase risk in any male injected with MMR before 36 months of age. Guess which racial group has the highest incidence of autism? If you guessed African American males, you win the prize. Guess who suffers with more autism, boys or girls? If you guessed boys, you win again.

Mia, left paralyzed from the neck down after suffering a reaction to the HPV vaccine, has no feeling in her arms or legs and is unable to lift her head. Her Mother, Gini Blesky, says the symptoms of her debilitating illness all began after being given Gardasil. Parents! Please BE INFORMED now and share this crucial information with everyone you love. View this newly available docu-series right now and protect your beloved children: tinyurl.com/VaccinationEducation#Gardasil #Cervarix #RevolutionForChoice #HearThisWell #VaccineInjury #VAXXED #INFORMEDconsent

Johns Hopkins Researcher Releases Shocking Report On Flu Vaccines
In 2015, a whole new slew of flu vaccines found themselves getting approved by the Federal Drug Administration. This isn’t an uncommon practice; most flu vaccines pass inspection every year. It’s well known advice that has been passed down from doctor to patient that the flu vaccine is something that we all should get, but it has been quickly surfacing that what’s in the vaccines–especially those from 2015 and after–might actually be more damaging then simply rolling the dice on getting the flu.
The ingredient that is getting the most flack is called an adjuvant. The particular one involved is called Squalene, and it has been linked to auto-immune disease side effects. In fact, it may have been used during chemical attacks in the Gulf War. Symptoms include chronic fatigue, muscle aches, and neurologic damage.
While it may be a contested subject, it remains that we aren’t really sure what’s going into these vaccines we’re being convinced should be used. A scientist who has been working at the Johns Hopkins School of Medicine, released a report sharing his views on the subject. And they aren’t pretty.
Here is an excerpt from yournewswire.com that summarizes aspects of Peter Doshi’s report. You can find the original report at the British Medical Journal’s site. Determine for yourself if the evidence he presents is credible or not…

INFERTILITY – DISEASE – DEATH … Laura Hayes, Mother of vaccine-injured children, on a mission to end the vaccine holocaust! Share this LIFE-SAVING information with your loved ones and stay informed with this groundbreaking docu-series happening now: tinyurl.com/VaccinationEducation
“Would you allow something that could cause infertility, such as nonstick chemicals and solvents, to be injected into your child? Of course not. You know that you would never want to destroy your child’s future reproductive capabilities. However, millions of mothers across America are allowing doctors to inject their children with polysorbate 80, known to adversely affect fertility. And who knows what propylene glycol (antifreeze), Triton X100 (detergent), aluminum, mercury, foreign DNA fragments, and the myriad other vaccine ingredients do to one’s future reproductive ability, especially when injected in conjunction with polysorbate 80.
We know that the HPV vaccine has caused Primary Ovarian Failure (which is premature menopause) and amenorrhea (the prolonged cessation of a female’s menstrual cycle) in girls and young women, rendering them infertile, and possibly sterile for life. We know that tetanus vaccines given to girls and women in Kenya were laced with Human Chorionic Gonadotropin (HCG), rendering them sterile. How? Administering HCG via vaccination stimulates the production of antibodies to HCG, and these antibodies then cause the woman’s body to reject embryos, effectively sterilizing her. Such an HCG-laced tetanus vaccine is in actuality a contraception vaccine.
Do you think any of these Kenyan women was told that prior to vaccination? To add to the evilness and deception, the Kenyan women were given a 5-dose tetanus program spread over a number of years, versus the 2-3 dose norm. Clearly, those vaccines were being used for induced sterility and birth control without the girls’ and women’s knowledge or consent.
Does any parent or vaccine recipient really know what is in the vaccines being injected into their child or themselves? It’s no wonder pharmaceutical companies don’t test to see whether or not their vaccine products cause infertility, they already know the answer. Instead, they simply write “not tested for impairment of fertility” on their package inserts, and our unethical government regulators let them get away with that. Interestingly, we are seeing record numbers of couples struggling with infertility issues. Coincidence?
Would you allow something that could kill your baby to be injected into your otherwise healthy child? Of course not! Mothers would lay down their lives for their children, they don’t purposefully put them in harm’s way. However, millions of mothers across America are allowing doctors to inject their children with more and more vaccines, not knowing that each and every one carries the risk of death, even more so when combined, as they most often are.
Interestingly, we are seeing record numbers of babies who are dying before their 1st birthday in the U.S., including many of “SIDS” and “SBS” (the labels that unethical doctors and unethical medical examiners use for vaccine-induced deaths instead of calling them what they are…i.e. vaccine-induced deaths). Coincidence?
Now that we have discussed what is actually in vaccines, let’s talk once more about how parental instincts have been demeaned, grossly manipulated, and obliterated, specifically, about how parents have been grievously lied to and misled, to the point where parents are now allowing things that simply do not make sense.
Imagine looking from the outside in, and seeing a tiny newborn, small infant, or trusting toddler, being held down, painfully stuck with a needle multiple times, screaming so that its face is beet red with tears, all while the child’s parents not only watch, but due to being lied to and coerced, they participate in this atrocity! What must this do to the psyche and stress hormones of a child to have this happen, time and again, while the person he trusts most is not only allowing it, but participating in it?
What would you say if you walked by the window to my house, peered in, and saw my husband and me holding down our tiny baby on the dining room table, then roughly jabbing and injecting it multiple times with toxic cocktails and true witches’ brews of ingredients…all while our baby, or child of any age, screamed bloody murder, trying to escape our grip and savagery? I imagine you would whip out your cell phone, call the police, then try to barge into our home to stop the abuse! How is what I just described any different than what goes on every minute of every day in doctors’ offices and hospitals in our country and across the world? To be very clear, it isn’t.
To state it very plainly, vaccination is child abuse in the form of medical assault and battery. With regard to adults, when vaccination is carried out against one’s will or wishes, say for school admittance, job requirements, elder care and housing, or military admission, or when carried out with one who is hesitant, or with one who is unsuccessful in resisting and refusing, it also meets the legal definition for assault and battery.
We must begin to label these vaccine atrocities for what they are: blatant and inexcusable child abuse; medical assault and battery; and when death is the result for the vaccine recipient, involuntary manslaughter. These vaccine-induced injuries, illnesses, and deaths are iatrogenic in nature, meaning they are caused by doctors and nurses. Vaccinations are crimes against humanity, and there is no time to mince words about this fact.”
This is a MUST SEE docu-series – totally free! tinyurl.com/VaccinationEducation#RevolutionForChoice #VaccineInjury #TheTruthAboutVaccines #VAXXED #Infertility

STUDY: Reality Trumping Establishment Vaccine “Facts”
The past week has offered glimpses of hope for the growing number of people who know they are being lied to by the mainstream medical establishment about vaccine safety. More people are now aware that the kind of rigorous testing required for drugs to be put on the market does not apply to vaccines, or that vaccines like the HPV shot were not properly tested against a saline placebo before approval by the US Food and Drug Administration (FDA).
Yet, the medical establishment continues to omit these facts and instead focuses on why vaccine hesitancy is on the rise. Studies are being done in an attempt to understand vaccine hesitancy and come up with solutions to the “problem” of poor vaccine uptake. In 2014, the Boston Globe ran the headline Doctors Still Hesitant to Urge HPV Vaccine for Teenagers, highlighting a survey from the US Centers for Disease Control and Prevention (CDC), in which the agency stated that the inoculation rate is ‘unacceptably low.’ In 2015, NPR ran the story titled Doctors, Not Parents, Are the Biggest Obstacle to the HPV Vaccine in response to a study published in the journal Cancer Epidemiology, Biomarkers & Prevention, which found that more than a quarter of pediatricians and family doctors do not strongly endorse the HPV vaccine.
A new study in the journal PLOS One titled Misinformation Lingers in Memory: Failure of Three Pro-vaccination Strategies is an eye-opener at how clueless the medical establishment appears to be as to why its vaccine propaganda is being rejected. In this study, the researchers compared three strategies in vaccine promotion: a) contrasting myths vs. “facts,” b) employing “fact” and icon boxes, and c) showing images of non-vaccinated sick children. It should be noted that when the study’s authors refer to “facts,” they are using the term to mean vaccine propaganda. Beliefs in the autism-vaccine link and in vaccines side effects, along with intention to vaccinate a future child, were evaluated both immediately after the “correction intervention” and after a 7-day delay to reveal possible backfire effects. The study concluded the following:
“Results show that existing strategies to correct vaccine misinformation are ineffective and often backfire, resulting in the unintended opposite effect…”

Study – The Introduction of Diphtheria-Tetanus-Pertussis and Oral Polio Vaccine Among Young Infants in an Urban African Community: A Natural Experiment
Highlights
•When DTP and OPV were introduced in Guinea-Bissau in 1981, allocation by birthday resulted in a natural experiment of being vaccinated early or late.
•Between 3 and 5 months of age, children who received DTP and OPV early had 5-fold higher mortality than still unvaccinated children.
•In the only two studies of the introduction of DTP and OPV, co-administration of OPV with DTP may have reduced the negative effects of DTP.
Few studies have examined what happened to child survival when DTP and OPV were introduced in low-income countries. These vaccines were introduced in 1981 in an urban community in Guinea-Bissau from 3 months of age in connection with 3-monthly weighing sessions. Children were therefore allocated by birthday to receive vaccines early or late between 3 and 5 months of age. In this natural experiment vaccinated children had 5-fold higher mortality than not-yet-DTP-vaccinated children. DTP-only vaccinations were associated with higher mortality than DTP + OPV vaccinations. Hence, DTP may be associated with a negative effect on child survival.
Results
Among 3–5-month-old children, having received DTP (±OPV) was associated with a mortality hazard ratio (HR) of 5.00 (95% CI 1.53–16.3) compared with not-yet-DTP-vaccinated children. Differences in background factors did not explain the effect. The negative effect was particularly strong for children who had received DTP-only and no OPV (HR = 10.0 (2.61–38.6)). All-cause infant mortality after 3 months of age increased after the introduction of these vaccines (HR = 2.12 (1.07–4.19)).
Conclusion
DTP was associated with increased mortality; OPV may modify the effect of DTP.

Dr. Buchwald testimony before the Quebec College of Physicians Medical Board:Dr. Gerhard Buchwald takes the stand
A physician from Germany, Dr. Buchwald testifies through an interpreter. Dr. Lanctot tables his credentials as well as a copy of his book entitled “Vaccination: Business Based on Fear”. He is recognized as an expert on vaccination by the Committee.
Dr. Buchwald testifies that his experience includes being a medical counselor to an association of parents whose children have been injured or killed by vaccinations. He adds that he is aware of a thousand vaccination related injury cases and has had personal contact with 350 cases. In 150 of these cases, he wrote the medical opinion and acted as an advisor during the legal proceedings.
Dr Lanctot (L).: If you take this stand in your country, have you been reprimanded by the medical authorities?
B.: I wrote a paper entitled, “Vaccinations: A Crime Against our Children”. I received written reprimands from the College of Physicians… In Germany, we have a law called “Kronegesetz” in the Civil Code, which stipulates that everyone has the right to freely voice his or her opinion. When I was fed up with this nonsense with the College, I drew their attention to the fact that their responses were actually a breach of those sections of the law. German judges, who deal with these issues, are very touchy on this issue… It is impossible to suppress the free speech of a physician in a free country which is why the College knew that it would lose. They also knew that the press would really have a field day. Since then I’ve heard nothing more…
L.: You mentioned earlier that the first criterion in medicine is to do no harm… And you referred to these ethics in
He continues with a brief history of his experiences in general and describes how he got interested in the whole question of immunization. He recalls that after graduating from medical school, he was a supporter of vaccination policies, as was everyone else he knew. Then he relates to the Committee the story of the eldest of his three children, born in 1957, who at eighteen months received a smallpox vaccination and who, eight days later was no longer able to stand up in his crib. Until then, his son’s development had been absolutely normal:
“He fell sick with a post-vaccination encephalitis, and ever since, I have a completely destroyed human being at home.”
It was at that time that someone approached him to become a member of a protective association in Germany. It was through this group that he got to know other vaccination damage cases.

Study – Human papillomavirus vaccination and risk of autoimmune diseases: A large cohort study of over 2million young girls in France.
RESULTS:
Among 2,252,716 girls, 37% received HPV vaccine and 4,096 AID occurred during a mean follow-up time of 33months. The incidence of AID was not increased after exposure to HPV vaccination, except for Guillain-Barré syndrome (GBS) (incidence rate of 1.4 among exposed [20 cases] versus 0.4 per 100,000 PY among unexposed [23 cases]; adjusted HR: 3.78 [1.79-7.98]). This association persisted across numerous sensitivity analyses and was particularly marked in the first months following vaccination. Under the hypothesis of a causal relationship, this would result in 1-2 GBS cases attributable to HPV vaccine per 100,000 girls vaccinated.
CONCLUSIONS:
Our study provides reassuring results regarding the risk of AID after HPV vaccination, but an apparently increased risk of GBS was detected. Further studies are warranted to confirm this finding.

Study – Detection of contaminants in cell cultures, sera and trypsin.
Abstract
The aim of this study was standardization and application of polymerase chain reaction (PCR) for the detection of contaminants in cell cultures, sera and trypsin. Five PCR protocols were standardized to assess the presence of genetic material from mycoplasma, porcine circovirus 1 (PCV1), bovine leukemia virus (BLV) or bovine viral diarrhea virus (BVDV) in cell culture samples. PCR reactions for the genes GAPDH and beta-actin were used to evaluate the efficiency of nucleic acid extraction. The PCR protocols were applied to 88 cell culture samples from eight laboratories. The tests were also used to assess potential contamination in 10 trypsin samples and 13 fetal calf serum samples from different lots from five of the laboratories. The results showed the occurrence of the following as DNA cell culture contaminants: 34.1% for mycoplasma, 35.2% for PCV1, 23.9% for BVDV RNA and 2.3% for BLV. In fetal calf sera and trypsin samples BVDV RNA and PCV1 DNA was detected. The results demonstrated that cell culture, sera and trypsin used by different laboratories show a high rate of contaminants. The results highlight the need for monitoring cell cultures and controlling for biological contaminants in laboratories and cell banks working with these materials.

Vaccines-The True Weapons Of Mass Destruction
Dr.Rebecca Carley.
ADVERSE REACTIONS to immunizations are more common than many people realize.
Please visit her website: http://www.drcarley.com/

Biopersistence in the Brain of Aluminum Nanoparticles from Vaccines
Posted by Merinda Teller, Ph.D, MPH on Aug 14, 2017
In the 1990s, French clinicians and researchers began noticing and reporting on a mysterious inflammatory muscle disorder with a distinctive pathological pattern that later earned the name “macrophagic myofasciitis” or MMF.1 Myofasciitis refers to inflammation of muscles and their connective tissue (fascia).
Initially, the cause and features of MMF were unknown. Subsequent research by French investigators elucidated that the deltoid muscle lesions characteristic of MMF were secondary to intramuscular injection with vaccines containing aluminum hydroxide adjuvants.2 The lesions revealed both an ongoing local immune reaction along with long-term persistence of aluminum hydroxide at the injection site.2
An ongoing series of admirably methodical studies also have confirmed a number of other post-vaccination clinical symptoms associated with MMF.3 These disabling health problems include not just muscle pain but joint pain, chronic fatigue, autonomic nervous system dysfunction, autoimmunity, and cognitive dysfunction.4 The cognitive deficiencies experienced by MMF patients mirror the cognitive impairments that have been observed to result from chronic exposure to aluminum particles.5 Together, all of these dysfunctions are “paradigmatic” of an emerging aluminum-adjuvant-related syndrome that has come to be known as ASIA (autoimmune/inflammatory syndrome induced by adjuvants).

How Conflicts of Interest Have Corrupted the CDC
Story at-a-glance
Conflicts of interest have become more the rule than the occasional exception. Even the US Centers for Disease Control and Prevention (CDC) receives heavy funding from industry
A 2009 investigation by the Office of the Inspector General concluded the CDC has “a systemic lack of oversight of the ethics program”; 97 percent of disclosure forms filed by its advisors were incomplete
The editor-in-chief of the Lancet recently published a statement declaring that a lot of published research is unreliable at best; about half is completely false

Story at-a-glance
Book by investigative journalist reveals how the U.S. Centers for Disease Control and Prevention (CDC) has engaged in massive fraud, misinformation and manipulation of vaccine information
A Danish scientist hired by the CDC to investigate the vaccine-autism link was charged with 22 counts of fraud and theft, yet the U.S. has not bothered to extradite him from Denmark, where he can be easily found
Most doctors will tell you the science is settled; there’s no link between vaccines and autism. In reality, the CDC is well aware there’s a link. Suppression of such data is why so few doctors understand the problem

CDC Blocks Whistleblower From Vaccine Injury Testimony
Story at-a-glance
A 16-year-old boy with autism and his family are suing a medical clinic for administering vaccines they believe caused the boy’s autism
A key part of the case hinges on testimony from Dr. William Thompson, a research scientist at the U.S. Centers for Disease Control and Prevention (CDC) who claimed the CDC covered up a vaccine-autism connection in relation to the MMR vaccine
CDC director Thomas Frieden blocked the request to have Thompson testify, stating it “would not substantially promote the objectives of CDC”

HighWire with Del Bigtree
A new study proves we are winning! Are we over-vaccinating our pets? Controversial Veterinarian Dr. John Robb risks all; This and much more, on #HighWire with Del Bigtree. Thursdays at 11am @HighWireTalk @DelBigtree. http://www.protectthepets.com
#protectthepets #vaccineswork?
**watch the show here:**

Interview with Brandy Vaughan – Former Representative of the pharmaceutical company merck

Director of VAXXED responds to Australian authorities

A Two-Dose Vaccine For Chicken Pox Now Is Linked To An Epidemic Of Shingles
April 18, 2017 Dr. Brownstein
Dr. David Brownstein says that the two-dose vaccine for chicken pox does lower the rate of that childhood illness. However, shingles, which is a painful recurrence of chickenpox, mostly in adults, has become an epidemic that is directly related to the vaccine. Shingles is far more serious and life-threatening than chicken pox. The bottom line is that billions of dollars are spent on vaccinating children to reduce the rate of a relatively mild childhood disease only to make them more susceptible to the same virus as adults causing serious illness (more medical bills) and even death. Big Pharma wins at both ends of the cycle. –GEG

Vaccine Excipient & Media Summary
Excipients Included in U.S. Vaccines, by Vaccine
In addition to weakened or killed disease antigens (viruses or bacteria), vaccines contain very small amounts of other ingredients – excipients or media.

Australian Prime Minister and Wife Tied to Pharma, Pushing Mandatory Vaccination
Australia’s politicians are deeply tied to pharmaceutical corporations, the British Monarchy, and other corporate and institutional powers which threaten the freedom and prosperity of Australian citizens.
One product of this hegemony is Australia’s “No Jab No Pay” law, which strips welfare from citizens who refuse vaccination for themselves or their children.
You could say people should just go without government welfare, and that’s a good idea for participants in the philosophy of independence from the system (Voluntaryism or Agorism), but the “system” in Australia has been constructed to make it difficult for anyone who is left out.
They can use this as leverage to cut off other necessities from citizens who refuse vaccination.
Without regard for the world of evidence for why people should not vaccinate, politicians and mainstream media speak of “improving vaccination rates.”
In its full perspective, No Jab No Pay is an eventuality when you see who holds power in the country. Let’s start with the Australian Prime Minister, Malcolm Turnbull.
He’s a multi-millionaire, with a chairman of a pharma corporation (who works with Novartis and GlaxoSmithKline) for a wife.
According to Money Morning:
“Australia’s new prime minister is a wealthy man. Last night, much was made of the fact that he doesn’t need to be in public life to have power and financial reward. He’s already amassed quite a fortune. Even before he entered politics. Various sources estimate his net worth at between $180 million and $200 million.”
In the mid 90’s, Turnbull invested 500,000$ in OzEmail and returned with about $60 million.

Study – A vaccine that prevents pregnancy in women.
Abstract
We report here results of clinical trials on a birth control vaccine, consisting of a heterospecies dimer of the beta subunit of human chorionic gonadotropin (hCG) associated noncovalently with the alpha subunit of ovine luteinizing hormone and conjugated to tetanus and diphtheria toxoids as carriers, that induces antibodies of high avidity (K(a) approximately 10(10) M-1) against hCG. Fertile women exposed to conception over 1224 cycles recorded only one pregnancy at antibody titers of > 50 ng/ml (hCG bioneutralization capacity). The antibody response declines with time; fertility was regained when titers fell to < 35 ng/ml. This study presents evidence of the feasibility of a vaccine for control of human fertility.

The Dangerous Reasons You Should Never Give Your Baby Tylenol After Vaccines
The Blood Brain Barrier Faces Dangerous Vaccine Ingredients
Vaccines contain chemicals that are not beneficial for children of any age, especially for infants. You can read a list of vaccine ingredients here, as published by the CDC.
The list includes substances such as human DNA; squalene, a known cancer-causing adjuvant; thimerosal, a form of mercury known to cause neurological damage; aluminum; chick embryo cells; formaldehyde; and cell cultures from human embryos and guinea pigs.
Vaccines also contain excitotoxins, including monosodium glutamate (MSG), substances which can overstimulate and damage or even destroy brain cells, which would likely be even more dangerous to a still-developing brain.
All of these substance may cross the infant’s blood brain barrier. Sadly, babies’ blood brain barriers may be even more challenged when their parents give them popular pain relievers, such as acetaminophen, commonly known as Tylenol®.

The Risks of Mixing Tylenol with Vaccines
The CDC recently advised parents that giving children Tylenol pain relief after vaccination may make the vaccines less effective. The pain reliever’s ability to prevent fevers causes suppression of the immune system, which also renders the vaccines less effective. [9]
A 2011 report from the US Food and Drug Administration (FDA) warned parents and health care providers that overdoses of liquid acetaminophen in babies of children caused liver failure and death. [10]
Disturbingly, a recent research study demonstrated that increased use of acetaminophen during a child’s first year of life has been linked to higher rates of asthma. In addition, despite the unclear and complex causes of autism, the use of acetaminophen during infancy has also demonstrated a possible link to higher rates of autism. [11, 12]
The causes for these links are still unknown, but scientists have proposed that the use of acetaminophen may cause “alterations in glutathione levels.” Other leading theories include that the use of this popular pain reliever also causes “effects on serotonin, suppression of COX2, and specific effects of acetaminophen breakdown products.”
In simple terms, glutathione is a molecule made of three amino acids, the building blocks of life. Our bodies produce this vital substance naturally. It helps us stay healthy and prevent disease, aiding our bodies to fight cancer, heart disease, dementia, and chronic disease. As a supplement, it has been used to treat autism, Alzheimer’s disease, and cancer. [13]
When babies are vaccinated, many vaccine ingredients may cross the blood brain barrier. When parents give their babies pain relief in combination with a vaccine, glutathione levels may be lowered or depleted, preventing this important “security guard” from removing vaccine toxins from the brain and other parts of the body.
In addition, parents may be unable to recognize adverse reactions to vaccines because acetaminophen conceals crying, fevers, and other symptoms.

Conclusion
The widely accepted use of acetaminophen pain relievers, such as Tylenol, has been shown in scientific studies to deplete levels of our bodies’ master antioxidant, glutathione. Parents should question the popular notion that dozens of vaccine doses in infancy are safe, and they should certainly research the damaging effects acetaminophen can have on the developing brain.

Herd Immunity Theory Has Been Repeatedly Disproven
by Marco Cáceres
The Vaccine Reaction
Several years ago I wrote about the theory of “herd immunity” and explained why it is a myth when applied to a vaccinated population. The herd immunity theory was formulated based on observations during the early 20th century of how an infectious disease appeared to lose its capacity to infect and spread after more than half of the people in a community had been infected with the disease and developed natural, life-long immunity to that disease. [1]
The theory of herd immunity was never meant to be applied to a vaccinated population, but rather was co-opted later in the 20th century to help justify mass, mandatory vaccination campaigns to eliminate infectious diseases for the so-called “greater good.” Its validity was grounded on the underlying assumption that the herd was protected because a significant portion of that herd had become stronger as a result of the natural process of contracting and surviving an infection.
The more members of the herd (community), who were exposed to an infectious disease and developed natural immunity to it the less of a threat that disease posed to the entire herd (community).
This same concept does not work in a highly vaccinated population for one simple reason: Vaccination stimulates an artificial, temporary immunity that does not last as long as naturally acquired immunity. Sometimes vaccination does not prevent infection at all but allows infection with few or no symptoms in the vaccinated person, who is still able to transmit the infection to others, which is the case with B. pertussis (whooping cough). [2] At best, it may stave off infections in some vaccinated people for a limited period of time.
Consequently, a vaccinated herd is never really protected. There is an illusion of protection in such a scenario because those who have been vaccinated remain vulnerable to infection and, thus, so does the herd—vaccinated and unvaccinated alike.

Schoolgirls sent to hospital after getting HPV vaccine
WRITER: CHINNAWAT SINGHA
PHITSANULOK – Four Prathom 5 students were rushed to a hospital after they were given an HPV vaccination on Wednesday morning. Following the injection – said to help prevent the development of cervical…

1. In 2010 the FDA allowed a presentation by those injured by HPV Vaccines… they have still not responded.2. Since the introduction of HPV Vaccines, VAERS reports of autoimmune conditions have increased more than 1000%, infertility reports increased 790%, spontaneous abortion (miscarriage) reports increased 270%, blindness and deafness reports increased 188%.3. HPV Vaccines account for 25% of all VAERS reports.4. It costs the U.S. $30,000,000 per year in HPV vaccines to eliminate less than 3 deaths per 100,000 women from cervical cancer… which would have been caught by pap smears anyway. AND this is despite the fact that HPV vaccines do not prevent CIN1/2 lesions from progressing to CIN3.5. Merck has always promised there is no HPV viral DNA in HPV vaccines, which is an outright lie. In 2012, Dr. Lee found that 100% of all HPV Vaccines contain HPV Viral DNA, and this was confirmed by French scientists in 2014. Injecting HPV Viral DNA causes HPV infection.6. In 2015 it was discovered by an Australian scientist that Merck’s HPV Vaccine “saline placebo” was not saline. It was Polysorbate 80… which causes ovarian failure, infertility, autoimmunity and nut allergies. This is important because that means when comparing the vaccine (containing Polysorbate 80) to the placebo, they could confidently say there were no differences or changes. (Polysorbate 80 is an ingredient in numerous vaccines.)7. In 2015 Dr. Lee officially recommended no physical activity or sports for at least 2 months after receiving Gardasil because of the very high chance of cardiac arrest.